Mystery Behind Red Blood Cell Maturation Solved
Red blood cells are formed in the bone marrow from haematopoietic stem cells via a complex process known as erythropoiesis. Towards the end of this process, immature red blood cells also known as reticulocytes (multi-lobular and spherical) undergo dynamic re-arrangements to yield highly deformable biconcave erythrocytes (also known as normocytes), which performs gaseous and nutrient exchange throughout the body. However, molecular mechanisms underpinning these remarkable morphological and bio-mechanical transformations remained largely unknown. Through quantitative profiling of protein composition and imaging, a research team lead by Singapore University of Technology and Design (SUTD) Assistant Professor Rajesh Chandramohanadas is now able to explain this intriguing biological phenomenon.
Reticulocytes form a small proportion of human peripheral blood, often less than 2% of the total red blood cells. Therefore it is difficult to purify them in sufficient quantities and quality for large-scale experiments. To circumvent this problem, SUTD researchers purified young reticulocytes from cord blood (which contains ~ 4% reticulocytes) from normal term pregnancies. A magnetic selection protocol using an antibody against transferrin receptor was used to isolate immature red blood cells. To reduce sample complexity and increase overall coverage, these cells were again fractionated into membrane and soluble samples. Thereafter, a sophisticated quantitative mass spectrometry technique was employed which resulted in the identification and quantification of more than 1800 proteins. This is by far the most comprehensive information on protein composition for human red blood cells.
The team carefully analysed this large dataset and short-listed certain proteins such as talin and tubulin, which dramatically changed between immature and mature blood cells. Although such proteins are known to confer stiffness to biological cells, these proteins were confirmed as residues that remained in the reticulocytes from precursor cells.
The researchers then looked at the abundance of other proteins that are responsible for maintaining cellular architecture, such as a group of proteins called spectrins. Although the overall amount of spectrins remained comparable between reticulocytes and normocytes, the arrangement of these proteins were drastically different in reticulocytes as observed through microscopy. Filaments that formed spectrin-based network shrunk by roughly 20% during maturation, and this could account for the transition in shape and deformability of reticulocytes.
Principal investigator Prof Chandramohanadas said: "This robust dataset on the protein composition of human red blood cells could help promote understanding of pathological conditions that affect blood cell maturation and function. Furthermore, these results will facilitate targeted analysis of interactions between blood cells and infectious agents- such as Plasmodium vivax malaria parasites which only infect young human reticuocuytes."
This article has been republished from materials provided by Singapore University of Technology and Design. Note: material may have been edited for length and content. For further information, please contact the cited source.
Trang T. T. Chu, Ameya Sinha, Benoit Malleret, Rossarin Suwanarusk, Jung E. Park, Renugah Naidu, Rupambika Das, Bamaprasad Dutta, Seow Theng Ong, Navin K. Verma, Jerry K. Chan, François Nosten, Laurent Rénia, Siu K. Sze, Bruce Russell, Rajesh Chandramohanadas. Quantitative mass spectrometry of human reticulocytes reveal proteome-wide modifications during maturation. British Journal of Haematology, 2017; DOI: 10.1111/bjh.14976.
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